Preparation method for chiral intermediate for use in statins
a statin and intermediate technology, applied in the field of synthesis of pharmaceutical intermediates, can solve the problems of low overall yield and achieve the effects of low overall yield, high product quality, and high cost of synthesis
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example 1
ON AND SCREENING OF DIKETOREDUCTASE MUTANT
[0056]1. Site-Directed Saturation Mutagenesis of Diketoreductase (DKR) (SEQ ID NO: 7) Derived from Rhodococcus erythropolis SK121 Strain
[0057]The three-dimensional protein structure of the amino acid sequence of diketoreductase (DKR) was simulated on the website of Swiss-model, and the binding between the substrate and the protein was simulated by Docking, and the amino acids which may be correlated to the binding between the substrate and NAD and to NAD proton transfer were finally selected as mutant amino acids through Pymol analysis.
[0058]Based on mutant amino acids and the base sequences on both sides thereof (for the mutant amino acids, see the mutation sites in Table 1), corresponding mutant primers were designed with Primmer5.0 (Table 1). Using pET22b(+) expression vector comprising diketoreductase gene (purchased from Novagen, catalog No. 69744) as the template, complete linear segments were obtained through whole plasmid PCR. The ab...
example 2
ON OF THE CHIRAL INTERMEDIATE FOR USE IN STATIN DRUGS
(1) Synthesis of benzyloxyacetic acid (Compound 3)
[0065]960 g of tetrahydrofuran and 41 g of toluene were added into a reaction flask. While controlling the temperature of the system at 10-20° C., 534.0 g of potassium hydroxide was added in four portions. After the addition of potassium hydroxide was completed, 1371.1 g of benzyl alcohol was added into the system in three portions. 300.1 g of chloroacetic acid was dissolved in 480.5 g of tetrahydrofuran, and the solution of chloroacetic acid in tetrahydrofuran was added dropwise into the above system while maintaining the temperature at 70-80° C. The system was reacted until chloroacetic acid was completely consumed. After cooling the system down, 3.12 Kg of purified water was added and tetrahydrofuran was removed under reduced pressure. The aqueous phase was extracted four times with toluene, and adjusted with hydrochloric acid at 10-20° C. to pH 3. The aqueous phase was extracte...
example 3
ON OF THE CHIRAL INTERMEDIATE FOR USE IN STATIN DRUGS
(1) Synthesis of benzyloxyacetic acid (Compound 3)
[0081]720.3 g of tetrahydrofuran and 41.1 g of toluene were added into a reaction flask. While controlling the temperature of the system at 10-20° C., 382.1 g of sodium hydroxide was added in four portions. After the addition of sodium hydroxide was completed, 1371.1 g of benzyl alcohol was added into the system in three portions. 300.2 g of chloroacetic acid was dissolved in 720.5 g of tetrahydrofuran, and the solution of chloroacetic acid in tetrahydrofuran was added dropwise into the above system while maintaining the temperature at 70-80° C. The system was reacted until chloroacetic acid was completely consumed. After cooling the system down, 3.1 Kg of purified water was added and tetrahydrofuran was removed under reduced pressure. The aqueous phase was extracted four times with toluene, and adjusted with hydrochloric acid at 10-20° C. to pH 3.2. The aqueous phase was extracted...
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